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慢性锂治疗可调节心理社会应激与认知的分子特征。

Molecular Signatures of Psychosocial Stress and Cognition Are Modulated by Chronic Lithium Treatment.

作者信息

Brzózka Magdalena M, Havemann-Reinecke Ursula, Wichert Sven P, Falkai Peter, Rossner Moritz J

机构信息

Molecular and Behavioral Neurobiology, Department of Psychiatry, Ludwig-Maximillians-University, Munich, Germany;

Department of Psychiatry and CNMPB-DFG Research Center, Georg-August-University, Goettingen, Germany;

出版信息

Schizophr Bull. 2016 Jul;42 Suppl 1(Suppl 1):S22-33. doi: 10.1093/schbul/sbv194. Epub 2015 Dec 28.

Abstract

Chronic psychosocial stress is an important environmental risk factor of psychiatric diseases such as schizophrenia. Social defeat in rodents has been shown to be associated with maladaptive cellular and behavioral consequences including cognitive impairments. Although gene expression changes upon psychosocial stress have been described, a comprehensive transcriptome profiling study at the global level in precisely defined hippocampal subregions which are associated with learning has been lacking. In this study, we exposed adult C57Bl/6N mice for 3 weeks to "resident-intruder" paradigm and combined laser capture microdissection with microarray analyses to identify transcriptomic signatures of chronic psychosocial stress in dentate gyrus and CA3 subregion of the dorsal hippocampus. At the individual transcript level, we detected subregion specific stress responses whereas gene set enrichment analyses (GSEA) identified several common pathways upregulated upon chronic psychosocial stress related to proteasomal function and energy supply. Behavioral profiling revealed stress-associated impairments most prominent in fear memory formation which was prevented by chronic lithium treatment. Thus, we again microdissected the CA3 region and performed global transcriptome analysis to search for molecular signatures altered by lithium treatment in stressed animals. By combining GSEA with unsupervised clustering, we detected pathways that are regulated by stress and lithium in the CA3 region of the hippocampus including proteasomal components, oxidative phosphorylation, and anti-oxidative mechanisms. Our study thus provides insight into hidden molecular phenotypes of chronic psychosocial stress and lithium treatment and proves a beneficial role for lithium treatment as an agent attenuating negative effects of psychosocial stress on cognition.

摘要

慢性心理社会应激是精神分裂症等精神疾病的重要环境风险因素。啮齿动物的社会挫败已被证明与包括认知障碍在内的适应不良的细胞和行为后果有关。尽管已经描述了心理社会应激后基因表达的变化,但在与学习相关的精确定义的海马亚区域进行全面的全基因组转录组分析研究仍很缺乏。在本研究中,我们将成年C57Bl/6N小鼠暴露于“定居者-入侵者”范式3周,并将激光捕获显微切割与微阵列分析相结合,以确定背侧海马齿状回和CA3亚区域慢性心理社会应激的转录组特征。在个体转录水平上,我们检测到亚区域特异性应激反应,而基因集富集分析(GSEA)确定了在慢性心理社会应激后上调的几个与蛋白酶体功能和能量供应相关的共同通路。行为分析显示,应激相关损伤在恐惧记忆形成中最为突出,而慢性锂治疗可预防这种损伤。因此,我们再次对CA3区域进行显微切割,并进行全基因组转录组分析,以寻找应激动物中锂治疗改变的分子特征。通过将GSEA与无监督聚类相结合,我们在海马CA3区域检测到受应激和锂调节的通路,包括蛋白酶体成分、氧化磷酸化和抗氧化机制。因此,我们的研究为慢性心理社会应激和锂治疗的隐藏分子表型提供了见解,并证明锂治疗作为一种减轻心理社会应激对认知负面影响的药物具有有益作用。

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